Expression Genetics of CYP3A Drug Metabolizing Enzymes

CYP3A药物代谢酶的表达遗传学

• 批准号: 9901542
• 负责人: Danxin Wang
• 金额: $ 26.86万
• 依托单位: UNIVERSITY OF FLORIDA
• 依托单位国家: 美国
• 财政年份: 2017
• 资助国家: 美国
• 起止时间: 2017-04-01 至 2022-03-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/9901542
• 关键词: Accounting; Address; Affect; Architecture; Binding; Biological Markers; CYP2D6 gene; CYP3A4 gene; CYP7A1 gene; Chromatin; Chromatin Loop; Clinical; Clustered Regularly Interspaced Short Palindromic Repeats; Complex; Cytochromes; DNA Binding; Data; Disease; Distal; Down-Regulation; Drug Exposure; Drug usage; Enhancers; Enzymes; Epigenetic Process; Estrogen Receptor alpha; Expression Profiling; Female; Gene Activation; Gene Cluster; Gene Expression; Gene Expression Regulation; Gene Frequency; Gene Silencing; Genes; Genetic; Genetic Polymorphism; Genetic Transcription; Genetic Variation; Genomic Segment; Genomic approach; Genomics; Goals; Hepatic; Hepatocyte; Human; Introns; Knowledge; Liver; Mediating; Methodology; Methods; Mission; Modeling; Modification; Molds; Molecular Genetics; Nonlinear Dynamics; Nucleic Acid Regulatory Sequences; Pathway Analysis; Pharmaceutical Preparations; Pharmacogenomics; Pharmacotherapy; Population; Public Health; Publishing; RNA Splicing; Regulation; Regulatory Element; Research; Role; Technology; Transcriptional Regulation; Translating; Treatment outcome; United States National Institutes of Health; Up-Regulation; Variant; base; biomarker development; biomarker panel; causal variant; clinical biomarkers; clinical practice; drug metabolism; enzyme activity; functional genomics; genetic approach; genetic architecture; genetic variant; genome editing; genomic locus; genomic variation; indexing; innovation; insight; inter-individual variation; male; mathematical model; network models; non-genetic; novel; personalized therapeutic; precision drugs; predictive modeling; promoter; theories; therapy outcome; transcription factor; transcriptome

Summary/Abstract Drug exposure and therapeutic outcomes are greatly affected by substantial variability in drug metabolism. CYP3A drug metabolizing enzymes, encoded by four genes clustered into one gene locus (most important CYP3A4, and 3A5, 3A7 and 3A43), are abundant and clinically important, metabolizing nearly half of all current drugs. However, CYP3A enzyme expression displays substantial (>10-fold) inter-individual variability, largely of unknown causes and therefore poorly predictable – leading to suboptimal treatment outcomes. Built on novel concepts in functional genomics, this proposal focuses on the genomic architecture and transcription factor (TF) regulation of the CYP3A locus, applying cutting edge methodologies and novel mathematical modeling of regulatory networks. The goal is to identify the combined effect of all main regulatory factors determining highly variable CYP3A enzymes – a critical step toward guiding personalized therapeutics of a substantial portion of current drugs. Our central hypothesis is that long-range interactions between regulatory elements (e.g., enhancers with genetic variants) within the CYP3A locus and perturbation of the relevant TF network, i.e., the CYP3A interactome, account for much of variable CYP3A expression. Applying a comprehensive experimental and computational approach, we have already demonstrated the presence of yet unknown regulatory genetic variants in several new enhancer regions that are spread across the CYP3A locus and interact with each other (via DNA looping), strong support of the need to study the CYP3A locus as an interactome, rather than each gene in isolation. Similarly, we need to study TFs regulating CYP3A expression as a dynamic network – an approach already taken previously. However, using a novel mathematical modeling approach, we identify new key TFs and characterize their dynamic interactions. For example, our modeling predicts that the estrogen receptor alpha (ESR1) (in an unliganded form present in males and females) is a critical determinant of CYP3A4 expression in liver cells. Indeed, our genome-editing methods with CRISPR demonstrate that ESR1 exerts profound influence on CYP3A4 expression, possibly accounting for a substantial portion of variability. Since robust ESR1 genetic variation has been implicated in numerous diseases while the causative variants remain uncertain, this project (aim3) will focus on the molecular genetics of ESR1, with largely unknown functions in the liver. The proposed research is innovative in studying gene regulation of the whole CYP3A interactome rather than single genes, and employing a novel mathematical modeling approach capable of identifying TFs, such as ESR1, as key factors in molding local chromatin architecture. Collectively, the results are expected to advance the field of pharmacogenomics by revealing fundamental mechanisms regulating complex gene loci, broadly applicable to similar gene clusters. The results will account for a substantial portion of CYP3A variability, guiding biomarker development for CYP3A activity.

摘要/文摘

项目成果

ESR1 ChIP-Seq Identifies Distinct Ligand-Free ESR1 Genomic Binding Sites in Human Hepatocytes and Liver Tissue.

• DOI: 10.3390/ijms22031461
• 发表时间: 2021-02-02
• 期刊: International journal of molecular sciences
• 影响因子: 5.6
• 作者: Collins JM;Huo Z;Wang D
• 通讯作者: Wang D

Cis-acting regulatory elements regulating CYP3A4 transcription in human liver.

• DOI: 10.1097/fpc.0000000000000402
• 发表时间: 2020-07
• 期刊: Pharmacogenetics and genomics
• 影响因子: 2.6
• 作者: Collins JM;Wang D
• 通讯作者: Wang D